Sculier J P, Lafitte J J, Paesmans M, Thiriaux J, Alexopoulos C G, Baumöhl J, Schmerber J, Koumakis G, Florin M C, Zacharias C, Berghmans T, Mommen P, Ninane V, Klastersky J
Service de Médecine, For the European Lung Cancer Working Party, Institut Jules Bordet, 1 rue Héger-Bordet, Brussels, B-1000, Belgium.
Br J Cancer. 2000 Nov;83(9):1128-35. doi: 10.1054/bjoc.2000.1413.
A phase III randomized trial was conducted in patients with metastatic NSCLC, to determine if, in association with mitomycin (6 mg m(-2)) and ifosfamide (3 g m(-2)), the combination of moderate dosages of cisplatin (60 mg m(-2)) and carboplatin (200 mg m(-2)) - CarboMIP regimen - improved survival in comparison with cisplatin (50 mg m(-2)) alone - MIP regimen. A total of 305 patients with no prior chemotherapy were randomized, including 297 patients assessable for survival (147 in the MIP arm and 150 in the CarboMIP arm) and 268 patients assessable for response to chemotherapy. All but eight (with malignant pleural effusion) had stage IV disease. There was a 27% (95% CI, 19-34) objective response (OR) rate to MIP (25% of the eligible patients) and a 33% (95% CI, 24-41) OR rate to CarboMIP (29% of the eligible patients). This difference was not statistically significant (P = 0.34). Duration of response was not significantly different between both arms. There was also no difference (P = 0.67) in survival: median survival times were 28 weeks (95% Cl, 24-32) for MIP and 32 weeks (95% Cl, 26-35) for CarboMIP, with respectively 1-year survival rates of 24% and 23% and 2-year survival rates of 5% and 2%. The main toxicities consisted in emesis, alopecia, leucopenia and thrombocytopenia, that were, except alopecia, significantly more severe in the CarboMIP arm. Our trial failed to demonstrate a significant improvement in response or survival when patients with metastatic NSCLC were treated, in addition to ifosfamide and mitomycin, by combination of moderate dosages of cisplatin and carboplatin instead of moderate dosage of cisplatin alone. The results support the use of a moderate dose (50 mg m(-2)) of cisplatin in combination with ifosfamide and mitomycin for the chemotherapy of this disease.
对转移性非小细胞肺癌患者进行了一项III期随机试验,以确定与丝裂霉素(6mg/m²)和异环磷酰胺(3g/m²)联合使用时,中等剂量顺铂(60mg/m²)和卡铂(200mg/m²)的联合方案——卡铂MIP方案,与单独使用顺铂(50mg/m²)——MIP方案相比,是否能提高生存率。共有305例未接受过化疗的患者被随机分组,其中297例患者可评估生存率(MIP组147例,卡铂MIP组150例),268例患者可评估化疗反应。除8例(有恶性胸腔积液)外,所有患者均为IV期疾病。MIP方案的客观缓解(OR)率为27%(95%CI,19 - 34)(占 eligible 患者的25%),卡铂MIP方案的OR率为33%(95%CI,24 - 41)(占 eligible 患者的29%)。这种差异无统计学意义(P = 0.34)。两组的缓解持续时间无显著差异。生存率也无差异(P = 0.67):MIP组的中位生存时间为28周(95%CI,24 - 32),卡铂MIP组为32周(95%CI,26 - 35),1年生存率分别为24%和23%,2年生存率分别为5%和2%。主要毒性包括呕吐、脱发、白细胞减少和血小板减少,除脱发外,卡铂MIP组的这些毒性明显更严重。我们的试验未能证明,对于转移性非小细胞肺癌患者,除异环磷酰胺和丝裂霉素外,联合使用中等剂量的顺铂和卡铂而非单独使用中等剂量的顺铂进行治疗,在反应或生存方面有显著改善。结果支持使用中等剂量(50mg/m²)的顺铂联合异环磷酰胺和丝裂霉素用于该疾病的化疗。